AI Article Synopsis

  • Platinum is commonly used in treating childhood cancers, but it can cause significant hearing loss (ototoxicity) in patients.
  • Research indicates that genetic factors may help identify which children are at greater risk for developing ototoxicity when treated with platinum-based drugs like cisplatin and carboplatin.
  • A study found that specific gene polymorphisms and higher cumulative doses of carboplatin correlated with an increased likelihood of hearing loss in pediatric patients, suggesting these genetic markers could be useful in predicting risk.

Article Abstract

Platinum is extensively used in the treatment of several childhood cancers. However, ototoxicity is one of the most notable adverse effects, especially in children. Several studies suggest that genetics may predict its occurrence. Here, polymorphisms associated with platinum-induced ototoxicity were selected from the literature and were investigated in a pediatric population treated with platinum-based agents. In this retrospective study, patients treated with cisplatin and/or carboplatin were screened. The patients with pre- and post-treatment audiogram (Brock criteria) available were included. We selected polymorphisms that have previously been associated with cisplatin ototoxicity with a minor allele frequency ≥30%. Deletion of and , rs1799735 (), rs1695 (), rs4880 (), rs2228001 (), rs1799793 () and rs4788863 () were investigated. Data of one hundred and six children matching the eligible criteria were analyzed. Thirty-three patients (31%) developed ototoxicity (with a Brock grade ≥2). The probability of hearing loss increased significantly in patients carrying the null genotype for (P = 0.03), A/A genotype at rs1695 (P = 0.01), and C/C genotype at rs1799793 (P = 0.008). We also showed an association of the cumulative doses of carboplatin with cisplatin ototoxicity (P <0.05). To conclude, deletion of , rs1695 and rs1799793 may constitute potential predictors of platinum-induced ototoxicity.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6089394PMC
http://dx.doi.org/10.18632/oncotarget.25767DOI Listing

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